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Fig. 5

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ZDB-IMAGE-120816-7
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Figures for Provost et al., 2012
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Fig. 5 Knockdown of rpl3 phenocopies SbdsATG MO-induced defects in pancreas development. (A) Expression of rpl3 is widespread at 24 hpf and becomes progressively restricted to the endoderm, with high-level pancreatic expression at 120 hpf. The principal islet (I) is labeled by in situ hybridization for insulin (red). (B) rpl3 expression is decreased in SbdsATG MO-injected embryos, as quantified by microarray analysis of transcript abundance. Error bars indicate s.e.m. (C) In situ hybridization for rpl3 in SbdsATG MO-injected p53zdf1/zdf1 embryos confirms loss of rpl3 expression in somites (black arrows), central nervous system (white arrows), pharyngeal arches (red arrows) and intestine (yellow arrows) of developing embryos. (D) An MO dose-dependent defect in pancreas progenitor expansion was observed in Rpl3ATG MO-injected ptf1a:eGFP;ins:mCherry;p53zdf1/zdf1 embryos. (E) The small pancreas (arrow) of p53zdf1/zdf1 embryos injected with 0.5 ng Rpl3ATG MO is positive for trypsin expression by in situ hybridization. (F) p53zdf1/zdf1 embryos injected with 0.5 ng Rpl3ATG MO at 72 hpf exhibit small heads and hydroencephaly (yellow arrowhead). (G) rpl3hi2437/+;ptf1a:eGFP;ins:mCherry heterozygotes bearing a mutagenic rpl3 transgenic insertion were incrossed. rpl3hi2437/hi2437 homozygous embryos displayed disrupted pancreas progenitor expansion at 72 hpf. Injection of rpl3hi2437;ptf1a:eGFP;ins:mCherry with the p53ATG MO did not rescue the pancreatic progenitor phenotype of homozygous rpl3hi2437hi/2437 embryos. L, liver; P, pancreas; I, islet; Ex, exocrine pancreas.

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